Multicenter retrospective study of patients with PCDH19‐related epilepsy: The first Hungarian cohort

癫痫 原钙粘蛋白 智力残疾 儿科 队列 回顾性队列研究 医学 队列研究 精神科 内科学 生物 遗传学 钙粘蛋白 细胞
作者
Mónika Kovács,András Fogarasi,Márta Hegyi,Zsuzsanna Siegler,Anna Kelemen,Mónika Mellár,Anna Orbok,Gábor Simon,Kristof Mark Farkas,Mónika Bessenyei,Katalin Hollódy
出处
期刊:Epileptic Disorders [Wiley]
卷期号:26 (5): 685-693
标识
DOI:10.1002/epd2.20264
摘要

Abstract Objective PCDH19‐related epilepsy occurs predominantly in girls and is caused by pathogenic variant of the protocadherin‐19 gene. The initial seizures usually develop in association with fever, begin on average at 15 months of age, and often occur in clusters. Autistic symptoms, intellectual disability, and sleep disturbance are often associated. Methods In our retrospective, multicenter study, we reviewed clinical data of nine children with epilepsy genetically confirmed to be associated with PCDH19. Results In the Hungarian patient population aged 0–18 years, the prevalence of PCDH19‐related epilepsy was found to be lower (1/100000 live births in females) than the reported international data (4–5/100000 live births in females). Four of our nine patients had positive family history of epilepsy (cousins, sister, and mother). We assessed brain anomalies in three patients (in one patient focal cortical dysplasia and left anterior cingulate dysgenesis, and in two children right or left hippocampal sclerosis) and in another three cases incidentally identified benign alterations on brain MRI were found. The first seizure presented as a cluster in seven out of nine children. In seven out of nine cases occurred status epilepticus. Six out of nine children had autistic symptoms and only one child had normal intellectual development. Seven of our patients were seizure free with combined antiseizure medication (ASM). The most effective ASMs were levetiracetam, valproate, and clobazam. Significance The prevalence of PCDH19‐related epilepsy is presumably underestimated because of the lack of widely performed molecular genetic evaluations. Molecular genetic testing including PCDH19 pathogenic variants is recommended for female patients with an onset of seizures before the age of 3 years.
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